Translational readthrough of ciliopathy genes BBS2 and ALMS1 restores protein, ciliogenesis and function in patient fibroblasts

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RESEARCH PRODUCT

Translational readthrough of ciliopathy genes BBS2 and ALMS1 restores protein, ciliogenesis and function in patient fibroblasts

Helen May-simera Jonathan Eintracht Elizabeth Forsythe Elizabeth Forsythe Mariya Moosajee

subject

BBS2 Adult Male Medicine (General)Adolescent Nonsense mutation Aminopyridines Cell Cycle Proteins Ciliopathies General Biochemistry Genetics and Molecular Biology chemistry.chemical_compound R5-920 Ataluren Ciliogenesis medicine Humans Receptors Somatostatin Bardet-Biedl Syndrome Alstrom Syndrome Cells Cultured Oxadiazoles business.industry Tumor Suppressor Proteins Translational readthrough R Proteins General Medicine Fibroblasts medicine.disease Nonsense suppression Ciliopathies Ataluren Ciliopathy ALMS1 chemistry Codon Nonsense Amlexanox Cancer research Medicine BBS2 business Alström syndrome Research Paper

description

Abstract Background Ciliary dysfunction underlies a range of genetic disorders collectively termed ciliopathies, for which there are no treatments available. Bardet-Biedl syndrome (BBS) is characterised by multisystemic involvement, including rod-cone dystrophy and renal abnormalities. Together with Alstrom syndrome (AS), they are known as the ‘obesity ciliopathies’ due to their common phenotype. Nonsense mutations are responsible for approximately 11% and 40% of BBS and AS cases, respectively. Translational readthrough inducing drugs (TRIDs) can restore full-length protein bypassing in-frame premature termination codons, and are a potential therapeutic approach for nonsense-mediated ciliopathies. Methods Patient fibroblasts harbouring nonsense mutations from two different ciliopathies (Bardet-Biedl Syndrome and Alstrom Syndrome) were treated with PTC124 (ataluren) or amlexanox. Following treatment, gene expression, protein levels and ciliogenesis were evaluated. The expression of intraflagellar transport protein IFT88 and G-protein coupled receptor SSTR3 was investigated as a readout of ciliary function. Findings mRNA expression was significantly increased in amlexanox-treated patient fibroblasts, and full-length BBS2 or ALMS1 protein expression was restored in PTC124- and amlexanox-treated fibroblasts. Treatment with TRIDs significantly improved ciliogenesis defects in BBS2Y24*/R275* fibroblasts. Treatment recovered IFT88 expression and corrected SSTR3 mislocalisation in BBS2Y24*/R275* and ALMS1S1645*/S1645* fibroblasts, suggesting rescue of ciliary function. Interpretation The recovery of full-length BBS2 and ALMS1 expression and correction of anatomical and functional ciliary defects in BBS2Y24*/R275* and ALMS1S1645*/S1645* fibroblasts suggest TRIDs are a potential therapeutic option for the treatment of nonsense-mediated ciliopathies. Funding Wellcome Trust 205174/Z/16/Z, National Centre for the Replacement, Refinement & Reduction of Animals in Research. Deutsche Forschungsgemeinschaft SPP2127 (DFG Grant MA 6139/3-1).

year	journal	country	edition	language
2021-08-01	EBioMedicine

10.1016/j.ebiom.2021.103515 http://europepmc.org/articles/PMC8353411